A Role for IL-27 in Limiting T Regulatory Cell Populations

Elia D. Tait Wojno; Nancy Hosken; Jason S. Stumhofer; Aisling O’Hara; Elizabeth A. Mauldin; Qun Fang; Laurence A. Turka; Steven D. Levin; Christopher A. Hunter

doi:10.4049/jimmunol.1004182

A Role for IL-27 in Limiting T Regulatory Cell Populations

Elia D. Tait Wojno(University of Pennsylvania), Nancy Hosken(Immungenetics (Germany)), Jason S. Stumhofer(University of Pennsylvania), Aisling O’Hara(University of Pennsylvania), Elizabeth A. Mauldin(University of Pennsylvania), Qun Fang(University of Pennsylvania), Laurence A. Turka(Beth Israel Deaconess Medical Center), Steven D. Levin(Immungenetics (Germany)), Christopher A. Hunter(University of Pennsylvania)

The Journal of Immunology

May 28, 2011

10.4049/jimmunol.1004182

Cited by 97Open Access

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Abstract

IL-27 is a cytokine that regulates Th function during autoimmune and pathogen-induced immune responses. Although previous studies have shown that regulatory T cells (Tregs) express the IL-27R, and that IL-27 inhibits forkhead box P3 upregulation in vitro, little is known about how IL-27 influences Tregs in vivo. The studies presented in this article show that mice that overexpress IL-27 had decreased Treg frequencies and developed spontaneous inflammation. Although IL-27 did not cause mature Tregs to downregulate forkhead box P3, transgenic overexpression in vivo limited the size of a differentiating Treg population in a bone marrow chimera model, which correlated with reduced production of IL-2, a vital cytokine for Treg maintenance. These data identify an indirect role for IL-27 in shaping the Treg pool.

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